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MR COLONOGRAPHY AND COLORECTAL CANCER

MR COLONOGRAPHY AND COLORECTAL CANCER. IOANNA TZOVARA,MD RADIOLODIST IASO GENERAL HOSPITAL ATHENS,GREECE. COLORECTAL CANCER. 2 nd most common Ca-related cause of death –major mortality The time from polyp to cancer development is approximately 10 years .

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MR COLONOGRAPHY AND COLORECTAL CANCER

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  1. MR COLONOGRAPHY AND COLORECTAL CANCER IOANNA TZOVARA,MD RADIOLODIST IASO GENERAL HOSPITAL ATHENS,GREECE.

  2. COLORECTAL CANCER • 2nd most common Ca-related cause of death –major mortality • The time from polyp to cancer development is approximately 10 years. • Early diagnosis of colorectal Ca is important due to the long natural course of the disease. Detection and treatment of adenomatous polyps that have not transformed into Ca yet and early localized Ca are possible through screening programs.

  3. SCREENING TOOLS • Fecal occult blood tests (FOBT) • Barium double-contrast enema • Colonoscopy (gold standard)

  4. VIRTUAL COLONOSCOPY • Bowel cleansing and discomfort of the Colononoscopyprocedures lead to poor patient acceptance and low screening rates for colonoscopy. • This led to the development of virtual colonoscopy, which includes both CT colonography and MR colonography. • From the late 1990s, more studies have been published about CT colonography than on MR colonography. • The CTC appears to be more suitable for colorectal screening than MR colonography.

  5. CT vs MR COLONOGRAPHY • CT colonography has several advantages reduced examination time fewer imaging artifacts higher spatial resolution wider availability less operator dependency lower cost. • However, a major advantage of MR colonography is the lack of ionizing radiation , a potential limitation of screening CT colonography.

  6. INDICATIONS F0R MRC • Indications for MR colonography Inflammatory bowel disease (IBD) Diverticulitis Assessment of colonic anastomoses Colorectal cancer screening Tortuous bowel Severe bowel spasm Extensive diverticular disease Incomplete colonoscopy due to obstructing tumor

  7. INDICATIONS • When a tumor occludes the colonic lumen, thereby preventing the colonoscope from being advanced more proximally, MR and CT colonography become very useful tools, since only air or liquid must pass through a stricture to allow visualization of the more proximal colon. • Synchronous lesions that otherwise would have been missed can be identified.

  8. MRC-CONTRAINDICATIONS • Before MR colonography, the patient must be screened for contraindications to MR imaging claustrophobia metallic implants cardiac pacemakers • Patients with hip prostheses are not ideal candidates for either MR colonography or CT colonography due to significant prosthesis-related artifact, which can obscure views of the rectum and sigmoid colon.

  9. PREPARATION Patients undegostandard bowel preparation with the same diet given by the gastroenterology endoscopy unit and take 3-4 liters of liquid food daily (water, tea, sour cherry juice, pudding, soup without fiber, and grain) for 2 days prior to the study. Patients take 210 mL of BT enema solution ) rectally and X-M Diet solution 250 mLperiorally1 day before the procedure; 210 mL of BT enema was repeated rectally on the morning of the procedure.

  10. PREPARATION The rigorous bowel preparation associated with colonoscopy and standard virtual colonoscopy remains one of the barriers to widespread acceptance of colorectal cancer screening.

  11. PREPARATION • Preparation-free or limited-preparation techniques have been used. • Similar to stool tagging in CT colonography, ingestion of oral tagging contrast material has been used in MR colonography to adapt the signal of stool to that of the enema fluid. • The results are promising, but further research is required to optimize the technique

  12. MRC PREPARATION • Conscious sedation and • Analgesia are unnecessary for MR colonography.

  13. MR COLONOGRAPHY • The most commonly used techniques are dark lumen and white lumen techniques. • In the dark lumen technique, water, air, or carbon dioxide is used in order to provide colon distention. Oral polyethylene glycol solution has been recently added to these techniques. • In the white lumen technique, a 1.5-2-L volume of gadolinium-containing enema is given via perioral or rectal route with 100-150 cm of hydrostatic pressure. So, the lumen shines with positive contrast medium,andis discriminated from the lesions

  14. BRIGHT AND DARK LUMEN • In MR colonography, the bright and dark-lumen strategy refers to the signal intensity of the bowel lumen at T1-weighted imaging. • In bright-lumen colonography, the bowel lumen is of high signal intensity and the colonic wall remains low in signal intensity. • Detection of colonic lesions is based on hypointense luminal filling defects with this approach. • Water spiked with paramagnetic contrast is used to distend the bowel lumen and to render the lumen bright. • Most bright-lumen MR colonography strategies only administer high-signal contrast material rectally • Added paramagnetic oral contrast agent to the major meals before MR colonography to tag fecal residue

  15. BRIGHT LUMEN MRC Potential false-positive filling defects, caused by air or residual stool .

  16. DARK LUMEN -PROCEDURE • Following rectal introduction of a 16F Foley catheter, the colon is gently filled with 2-2.5 l of warm tap waterfrom an enema bag held at shoulder height to distend the colon. Also used roomair and carbon dioxide • Bowel motility is abolished by intravenous spasmolytic(Buscopan; BoehringerIngelheim, Ingelheim, Germany) 0.3mg kg21 (max 20 mg) immediately prior to imaging • i.v. gadolinium (0.2mg /kg) is also administered.

  17. DARK LUMEN MRC Coronal gadolinium-enhanced T1-weighted spoiled GRE dark-lumen MR colonographic image shows a well-distended colon.

  18. DARK LUMEN MRC • The aim is to see the lesion by its enhancement in a dark lumen after intravenous contrast administration (Less false neg/pos) • Exam is completed in approximately 20-30 min after which the water is allowed to drain back into the enema bag. • While the cecum and ascending colon has the most artifacts, the fewest are found in the rectum. • The best distention is obtained in the rectum, and the worst is found in the cecum.

  19. GADOLINIUM ADMINIDTRATION • By measuring the signal intensities of the lesion on both pre-and postcontrast images, the amount of enhancement can be determined. • True colorectal lesions typically enhance, whereas residual stool particles do not.

  20. DRAWBACKS • Water filling experience. Cramps • Breath holding • Lying still in the MRI scanner (20min) • Scanner noise • Delay in the results interpretation

  21. 1.5 TESLA vs 3 TESLA • They found no significant difference in image quality at 1.5 T versus 3.0 T for polyps 6mm or larger

  22. MR COLONOGRAPHY • T2W coronal true fast imaging with steady-state precession (FISP) sequence • Axial T2-true-FISP • Axial T2 HASTE, • Diffusion-weighted images • 3D T1 vibe fat suppression coronal sequences • Gadolinium contrast medium administration intravenously. • T1 vibe fat suppression sequences were repeated on the axial and coronal planes.

  23. MRC PROCEDURE • A large phased-array coil is used to cover the complete abdomen. • For dark- and bright-lumen imaging, dual (prone and supine )positioning is recommended.

  24. IMAGE EVALUATION • MR colonography data should be evaluated on a workstation that allows for reconstruction of the 3D-acquired datasets. • 3D T1W sequences are used • 2D T2W sequences can be used for problem solving in cases of motion artifacts • Interpretation times are approximately 20 minutes

  25. IMAGE EVALUATION • An endoluminal fly-through should be performed whenever possible because it enables the radiologist to assess haustral morphologic characteristics more closely, allowing differentiation of haustra from true lesions. • It is recommended that both an antegrade and a retrograde fly-through be performed to allow visualization of both sides of the haustra.

  26. BRIGHT LUMEN MRC 10-mm polyp in sigmoid colon on a coronal T2-weighted true FISP image in a 64 year-old male patient with history of rectal hemorrhage and constipation. Verified on conventional colonoscopy. Histopathologic examination : hyperplasticpolyp

  27. DARK LUMEN MRC Polyp 10 mm detected in the sigmoid colon on T1W vibe fat suppression coronal post-contrast image analysis Verified on conventional colonoscopy In histopathologic examination : tubular adenomatous polyp

  28. MR COLONOGRAPHY Pedunculatedpolyp 20 mm in the lateral wall of the rectum on T1W post-contrast coronal image in a 27-year-old male patient with abdominal pain. Verified on conventional colonoscopy . Histopathologic examination: juvenile polyp

  29. MR COLONOGRAPHY Dark-lumen MRC of a 68-year-old male patient. Coronal 3D T1W turbo field-echo and 2D T2W single-shot turbo spin-echo demonstrated a contrast enhanced on T1W sequence mass lesion of 8 cm in the cecum, suspicious of colorectal cancer Colonoscopy : 4-cm mass lesion that was removed by hemicolectomy. Histopathology: poorly differentiated adenocarcinoma

  30. MRC Dark-lumen MRC of a 55-year-old male patient. Coronal 3D T1W and 2D T2W single-shot turbo spin-echo demonstrated a contrast enhanced on T1W sequence mass lesion of 4 cm in the ascending colon, suspicious of colorectal cancer Colonoscopy : 4-cm mass lesion Histopathology: adenocarcinoma

  31. MR COLONOGRAPHY Flat polyp. Axial and sagittal reformatted subtracted T1 W spoiled GRE images (subtraction of precontrast acquisition from 90-second postcontrast MR colonographic acquisition) show a 4-cm rectal mass that is minimally elevated above the colonic wall

  32. MR COLONOGRAPHY Three-dimensional (3D) T1W reconstruction in a 61-year-old female patient. Cor T1W turbo field-echo showed a small enhanced lesion in the middle of the lumen of the sigmoid over several image slices. Axial reconstruction clearly showed the stalk and head of a pedunculated polyp of 16 mm in the sigmoid. Colonoscopy : pedunculated polyp of 15 mm. Histopathology :Tubular adenoma.

  33. MRC-IBD Cor and ax 3D T1W turbo field-echo showed a stenotic segment of 6cm size with a prestenotic dilatation in the transverse colon of a 53-year-old female patient, suspected to be Crohn disease. Colon carcinoma could not be ruled out. Histopathology : stenotic segment with inflammatory activity caused by Crohn disease.

  34. MR COLONOGRAPHY • While a significant difference was not found between coronal true FISP and coronal T1 post-contrast sequences in terms of lesion detection sensitivity, coronal T1 pre-contrast analysis sensitivity was lower than other sequences. • Extracolonicfindings are also detected. Carrying prognostic value for the patient (37%) Findings (63%) have no prognostic values.

  35. MRC-EXTRACOLONIC FINDINGS Cor 2D T2W single-shot turbo spin-echo and coronal 3D T1W turbo field-echo demonstrated a mass lesion of 2.6cm in the right kidney of a 58-year-old male patient. Histopathology : renal cell carcinoma.

  36. Sensitivity of MR Colonography in the Detection of Colorectal Polyps and Masses Authors/Year of Study* Sequence No. of Patients No.of Polyps No. of Polyps Detected Overall ≤5 mm 6–10 mm ≥10 mm Sensitivity (%) Bright-lumen MRC Luboldt et al (2000) 3D T1W GRE 127 189 9/129 (7%) 19/31 (61%) 26/29 (90%)96 Pappalardo et al (2000) 3D T1W GRE 70 127 2/6 (33%) 29/30 (97%) 91/91 (100%) 95 Dark-lumen MRC Lauenstein and Debatin(2001) N/A 12 5 None 5/5 (100%) None 100 Ajaj et al (2003) 3D T1W GRE 122 50 0/30 (0%) 16/18 (89%) 2/2 (100%) 93 Hartmann et al (2006) 3D T1W GRE 92 07 4/44 (9%) 32/41 (78%) 22/22 (100%) 90 Ajaj et al (2006) 3D T1W GRE 72 90 0/65 (0%) 22/25† (88%) None 76 Saar et al (2008) 3D FLASH, 3D VIBE 34 24 4/8 (50%) 16/16 (100%) 4/4‡ (100%) N/A Limited bowel preparation Rodr Gomez et al(2008) 3D T1W GRE 83 56 0/36 (0%) 6/12 (50%) 8/8 (100%) N/A Kuehle et al (2007) 3D T1W GRE 315 235 16/153 (10%) 34/59 (58%) 17/23 (74%) 28.5 Achiam et al (2009) Uni 3D T1W GRE 56 89 5/66 (8%) 6/7 (86%) 13/16 (81%) N/A

  37. Pooled Per-Polyp Sensitivity of MR Colonographyfor Colorectal Polyp Detection by Size Sensitivity of Polyp Detection% Polyp Size No/Limited BP Standard BP Standard BP & Published after 2008 Large 82 (74–88) 89 (79–95) 95 (86–99) Medium-sized 70 (63–76) 81 (73–87) 80 (71–88) Large & med-sized 75 (70–79) 85 (79–89) 86 (80–90) Small 9 (6–13) 8 (5–13) 10 (6–17)

  38. MR COLONOGRAPHY • Sensitivity for the detection of CRC was 100%. • Significant heterogeneity was found for overall per patient sensitivity and specificity. • For polyps with a size of 10 mm or larger, per patient sensitivity and specificity estimates were 88% (95% CI 63–97%; I2=37%) and 99% (95% CI 95–100%; I2=60%). • On a per polyp basis, polyps of 10 mm or larger were detected with a sensitivity of 84% (95% CI 66–94%; I2=51%). • The data were too heterogeneous for polyps smaller than 6 mm (0-10%) and 6– 9 mm(50-80%). • Conclusion: MR-colonography can accurately detect colorectal polyps more than 10 mm in size

  39. Pooled Sensitivity of MR Colonography Compared With CT Colonography • MR colonography and CT colonography with 16-slice or 64-slice scanners have equal sensitivity for the detection of CRC, as well as for the detection of large and medium sized polyps; however, MR colonography does not carry the associated risks of ionizing radiation. • MR colonography and CT colonography with 16-slice or 64-slice scanners can reliably detect most CRCs and large colorectal polyps; however, about 20% of medium-sized colorectal polyps will be missed by both techniques. • None of the techniques can reliably detect small polyps and MR colonography has a much lower sensitivity for the detection of small polyps compared with CT colonography.

  40. MR COLONOGRAPHY • With the integration of 3.0-T MRcolonography, parallel imaging (an evolving data acquisition and reconstruction technique that makes use of coil arrays to encode and detect multiple data points simultaneously), • Fecal tagging (based on altering the signal intensity of feces by adding contrast material to patients’ meals in the days prior to MRC) • Fecal cracking e administration of stool softeners, both orally and rectally, which leads to hydration of stool and decrease in the signal intensity of stool in T1W imaging) • Nanoparticle-based MRC (an experimental method using solid lipid nanoparticles (SLNs) synthesized with loading gadolinium-DTPA to construct Gd-SLNs as an MR T1 contrast agent) methods into research and clinical settings, MRC gives us the hope of becoming a method that has higher detection ratios and easier clinical use.

  41. MR COLONOGRAPHY • In conclusion, MRC is a good alternative to other colorectal cancer screening methods: It is non-invasive, Has high sensitivity in colorectal lesions measuring 1 cm and above Enables assessment of extracolonicfindings and Does not include ionizing radiation. • Sensitivity may be increased by developing methods, like providing a good colonic cleaning and distention and reducing respiratory artifacts through good breathholding. • Future investigations by developing large-scale studies will likely lead to wider acceptance of this method to detect colonic pathologies, including perhaps their use in colon cancer screening programs.

  42. Thank you for your attention !

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